Antioxidant May Slow Parkinson’s

An analysis of data garnered from a two-decade-old trial has confirmed findings from a recent investigation that suggests the antioxidant urate may slow the progression of Parkinson’s disease.

Researchers analyzed blood and cerebrospinal fluid samples from a 1980s investigation of potential Parkinson’s medications and found evidence supporting the findings of their 2008 study on urate.

Investigators from MassGeneral Institute for Neurodegenerative Diseases (MGH-MIND) and Harvard School of Public Health (HSPH) have released their findings online and will publish their findings in the December Archives of Neurology.

“These results were critically important. Only now we can be reasonably sure that the slower rate of progression in patients with higher concentrations of urate is real and not a chance occurrence,” says Alberto Ascherio, MD, DrPh, of HSPH, the new study’s lead author.

Parkinson’s disease – characterized by tremors, rigidity, difficulty walking and other symptoms – is caused by destruction of brain cells that produce the neurotransmitter dopamine.

The 2008 study, which investigated the observation that healthy people with elevated but still normal urate levels have a reduced risk of developing Parkinson’s, found an association between higher blood urate levels and slower disease progression in 800 participants from a previous clinical trial.

To follow up that finding, the current study reviewed information from a much earlier trial that had investigated whether the drug deprenyl, now an established treatment for Parkinson’s, or doses of vitamin E would slow disease progression.

The researchers analyzed samples of both blood and cerebrospinal fluid from 800 participants in the DATATOP study, conducted by the Parkinson’s Study Group at centers across the U.S. and Canada, to find any association of urate levels with how quickly recently diagnosed patients progressed to the point where they needed to begin standard drug therapy.

Confirming the results of the 2008 study, they found that participants with the highest blood urate levels had a 36 percent less chance of needing to begin treatment during the two-year study period than did those with the lowest urate levels.

Similar results were seen for urate levels in the cerebrospinal fluid. Also echoing last year’s results, the association of urate levels with risk was robust in men but less clear in women, which may reflect the fact that few women have the high natural urate levels associated with risk reduction.

“Since cerebrospinal fluid circulates in and around the brain, the association with urate CSF levels strengthens the possibility that urate has a protective influence on the cells that degenerate in Parkinson’s disease,” says Michael Schwarzschild, MD, PhD, of MGH-MIND, the study’s senior author.

“Urate is a major antioxidant and it can protect brain cells in the lab, which makes this a compelling possibility; but we don’t yet know if it’s urate itself or some urate-determining factor that helps people with Parkinson’s.”

One unexpected observation was that the association of urate levels with disease progression was not seen in DATATOP trial participants who had received vitamin E, also a powerful antioxidant that had no effect on disease progression in the original study.

The researchers speculate that vitamin E might block urate’s effects or that the elevated doses in the DATATOP trial might have had a pro-oxidant effect, possibilities that need further investigation.

With the support of the Michael J. Fox Foundation, Schwarzschild and Ascherio, along with Parkinson Study Group colleagues from across the country, are conducting a multicenter Phase 2 trial at 10 centers. Enrolling 90 recently diagnosed patients, the SURE-PD trial will investigate whether treatment with the urate precursor inosine can safely increase urate levels with a goal of slowing disease progression.

“Because elevated urate levels have known health risks, including gout and kidney stones,” Schwarzschild stresses, “urate elevation should only be attempted in the context of a closely monitored clinical trial in which potential benefits and risks are carefully balanced.”

Last reviewed: By John M. Grohol, Psy.D. on 13 Oct 2009 Published on PsychCentral.com. All rights reserved.

About Rick Nauert PhD

Dr. Rick Nauert has over 25 years experience in clinical, administrative and academic healthcare. He is currently an associate professor for Rocky Mountain University of Health Professionals doctoral program in health promotion and wellness. Dr. Nauert began his career as a clinical physical therapist and served as a regional manager for a publicly traded multidisciplinary rehabilitation agency for 12 years. He has masters degrees in health-fitness management and healthcare administration and a doctoral degree from The University of Texas at Austin focused on health care informatics, health administration, health education and health policy. His research efforts included the area of telehealth with a specialty in disease management.